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Southampton University Medicine, Southampton General Hospital, Southampton SO16 6YD, United Kingdom
We have
investigated the effect of mechanical damage, cell density, and
cell-derived soluble mediators on CD44 expression in a model of
bronchial epithelial repair. CD44 (all isoforms) and variant-containing
isoforms (CD44v3, CD44v6, and CD44v9) were identified with flow
cytometry and immunocytochemistry with image analysis. After mechanical
damage, CD44 expression increased up to 500 µm from the wound edge
and for up to 48 h in two human bronchial epithelium-derived cell
lines, 16HBE14o
and NCI-H292. CD44 expression was unchanged by
interferon-
and increased by <50% by tumor necrosis factor-
.
To exclude other soluble factors, a Vaseline spacer was used to
temporarily divide petri dishes, with cells at high density on one side
and those at low density on the other. After the spacer was removed,
the cells at low cell density growing in the shared medium expressed up
to fourfold higher CD44, although cell proliferation was unchanged.
Thus increased CD44 expression at low cell density was not mediated by
soluble factors and may reflect functional involvement in cell
motility, dedifferentiation, or altered cell-substrate adhesion in
epithelial repair.
CD44 variants; bronchial epithelium; intercellular adhesion molecule-1; epithelial damage
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